Your search keyword '"Kwei, Kevin"' showing total 49 results

1. B-cell Receptor Pathway Mutations Are Infrequent in Patients with Chronic Lymphocytic Leukemia on Continuous Ibrutinib Therapy.

Author

Jones, Daniel, Cheung, Leo, Chong, Elizabeth, Kwei, Kevin, Dean, James, James, Danelle, Wiestner, Adrian, Woyach, Jennifer, Ghia, Paolo, Byrd, John, Ahn, Inhye, Moreno, Carol, and OBrien, Susan

Subjects

Humans, Leukemia, Lymphocytic, Chronic, B-Cell, Mutation, Agammaglobulinaemia Tyrosine Kinase, Receptors, Antigen, B-Cell

Abstract

PURPOSE: Acquired mutations in Brutons tyrosine kinase (BTK) or phospholipase C-γ2 (PLCG2) genes are associated with clinical progressive disease (PD) in patients with chronic lymphocytic leukemia (CLL) treated with BTK inhibitors. Data on mutation rates in patients without PD on ibrutinib treatment are limited. EXPERIMENTAL DESIGN: We evaluated frequency and time to detection of BTK and PLCG2 mutations in peripheral blood samples from 388 patients with previously untreated (n = 238) or relapsed/refractory (n = 150) CLL across five clinical trials. RESULTS: With median follow-up of 35 months (range, 0-72) without PD at last sampling, mutations in BTK (3%), PLCG2 (2%), or both genes (1%) were rare in previously untreated patients. With median follow-up of 35 months (range, 1-70) without PD at last sample, mutations in BTK (30%), PLCG2 (7%), or both genes (5%) were more common in patients with relapsed/refractory CLL. Median time to first detection of BTK C481S mutation was not reached in previously untreated patients and was >5 years in patients with relapsed/refractory CLL. Among patients evaluable at PD, previously untreated patients (n = 12) had lower rates than those with relapsed/refractory disease (n = 45) of BTK (25% vs. 49%) and PLCG2 mutations (8% vs. 13%). Time from first detection of BTK C481S mutation to PD was 11.3 months in 1 previously untreated patient and median 8.5 months (range, 0-35.7) among 23 patients with relapsed/refractory CLL. CONCLUSIONS: This systematic investigation describes development of mutations over time in patients without PD and informs the potential clinical opportunity to optimize ongoing benefits for such patients.

Published

2023

2. Durable ibrutinib responses in relapsed/refractory marginal zone lymphoma: long-term follow-up and biomarker analysis

Author

Noy, Ariela, de Vos, Sven, Coleman, Morton, Martin, Peter, Flowers, Christopher R., Thieblemont, Catherine, Morschhauser, Franck, Collins, Graham P., Ma, Shuo, Peles, Shachar, Smith, Stephen D., Barrientos, Jacqueline C., Chong, Elizabeth, Wu, Shiquan, Cheung, Leo W.-K., Kwei, Kevin, Hauns, Bernhard, Arango-Hisijara, Israel, and Chen, Robert

Published

2020

3. Data from B-cell Receptor Pathway Mutations Are Infrequent in Patients with Chronic Lymphocytic Leukemia on Continuous Ibrutinib Therapy

Author

Woyach, Jennifer A., primary, Ghia, Paolo, primary, Byrd, John C., primary, Ahn, Inhye E., primary, Moreno, Carol, primary, O'Brien, Susan M., primary, Jones, Daniel, primary, Cheung, Leo W.K., primary, Chong, Elizabeth, primary, Kwei, Kevin, primary, Dean, James P., primary, James, Danelle F., primary, and Wiestner, Adrian, primary

Published

2023

4. Supplementary Methods S1 from B-cell Receptor Pathway Mutations Are Infrequent in Patients with Chronic Lymphocytic Leukemia on Continuous Ibrutinib Therapy

Author

Woyach, Jennifer A., primary, Ghia, Paolo, primary, Byrd, John C., primary, Ahn, Inhye E., primary, Moreno, Carol, primary, O'Brien, Susan M., primary, Jones, Daniel, primary, Cheung, Leo W.K., primary, Chong, Elizabeth, primary, Kwei, Kevin, primary, Dean, James P., primary, James, Danelle F., primary, and Wiestner, Adrian, primary

Published

2023

5. Supplementary Table S1 from B-cell Receptor Pathway Mutations Are Infrequent in Patients with Chronic Lymphocytic Leukemia on Continuous Ibrutinib Therapy

Author

Woyach, Jennifer A., primary, Ghia, Paolo, primary, Byrd, John C., primary, Ahn, Inhye E., primary, Moreno, Carol, primary, O'Brien, Susan M., primary, Jones, Daniel, primary, Cheung, Leo W.K., primary, Chong, Elizabeth, primary, Kwei, Kevin, primary, Dean, James P., primary, James, Danelle F., primary, and Wiestner, Adrian, primary

Published

2023

6. B-cell Receptor Pathway Mutations Are Infrequent in Patients with Chronic Lymphocytic Leukemia on Continuous Ibrutinib Therapy

Author

Woyach, Jennifer A., primary, Ghia, Paolo, additional, Byrd, John C., additional, Ahn, Inhye E., additional, Moreno, Carol, additional, O'Brien, Susan M., additional, Jones, Daniel, additional, Cheung, Leo W.K., additional, Chong, Elizabeth, additional, Kwei, Kevin, additional, Dean, James P., additional, James, Danelle F., additional, and Wiestner, Adrian, additional

Published

2023

7. First-line treatment of chronic lymphocytic leukemia with ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab: final analysis of the randomized, phase 3 iLLUMINATE trial

Author

Hsu, Emily, Dai, Sandra, Kwei, Kevin, Gribben, John G, Strugov, Vladimir, Gill, Devinder, Novak, Jan, Simkovic, Martin, Larratt, Loree, Anz, Bertrand, Tedeschi, Alessandra, Greil, Richard, Moreno, Carol, Demirkan, FATİH, Flinn, Ian W, and Dean, James P

Published

2022

8. Identification of recurrent SMO and BRAF mutations in ameloblastomas

Author

Sweeney, Robert T, McClary, Andrew C, Myers, Benjamin R, Biscocho, Jewison, Neahring, Lila, Kwei, Kevin A, Qu, Kunbin, Gong, Xue, Ng, Tony, Jones, Carol D, Varma, Sushama, Odegaard, Justin I, Sugiyama, Toshihiro, Koyota, Souichi, Rubin, Brian P, Troxell, Megan L, Pelham, Robert J, Zehnder, James L, Beachy, Philip A, Pollack, Jonathan R, and West, Robert B

Published

2014

9. Genomic instability in breast cancer: Pathogenesis and clinical implications

Author

Kwei, Kevin A., Kung, Yvonne, Salari, Keyan, Holcomb, Ilona N., and Pollack, Jonathan R.

Published

2010

10. First-line treatment of chronic lymphocytic leukemia with ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab: final analysis of the randomized, phase III iLLUMINATE trial

Author

Moreno, Carol, primary, Greil, Richard, additional, Demirkan, Fatih, additional, Tedeschi, Alessandra, additional, Anz, Bertrand, additional, Larratt, Loree, additional, Simkovic, Martin, additional, Novak, Jan, additional, Strugov, Vladimir, additional, Gill, Devinder, additional, Gribben, John G., additional, Kwei, Kevin, additional, Dai, Sandra, additional, Hsu, Emily, additional, Dean, James P., additional, and Flinn, Ian W., additional

Published

2022

11. Up to 6.5 years (median 4 years) of follow-up of first-line ibrutinib in patients with chronic lymphocytic leukemia/small lymphocytic lymphoma and high-risk genomic features: integrated analysis of two phase 3 studies

Author

Burger, Jan A., primary, Robak, Tadeusz, additional, Demirkan, Fatih, additional, Bairey, Osnat, additional, Moreno, Carol, additional, Simpson, David, additional, Munir, Talha, additional, Stevens, Don A., additional, Dai, Sandra, additional, Cheung, Leo W. K., additional, Kwei, Kevin, additional, Lal, Indu, additional, Hsu, Emily, additional, Kipps, Thomas J., additional, and Tedeschi, Alessandra, additional

Published

2022

12. CAMK1D amplification implicated in epithelial–mesenchymal transition in basal-like breast cancer

Author

Bergamaschi, Anna, Kim, Young H., Kwei, Kevin A., La Choi, Yoon, Bocanegra, Melanie, Langerød, Anita, Han, Wonshik, Noh, Dong-Young, Huntsman, David G., Jeffrey, Stefanie S., Børresen-Dale, Anne-Lise, and Pollack, Jonathan R.

Published

2008

13. Phase 1b/2 study of ibrutinib and lenalidomide with dose-adjusted EPOCH-R in patients with relapsed/refractory diffuse large B-cell lymphoma*

Author

Wilson, Wyndham H., primary, Phillips, Tycel, additional, Popplewell, Leslie, additional, de Vos, Sven, additional, Chhabra, Saurabh, additional, Kimball, Amy S., additional, Beaupre, Darrin, additional, Huang, Da Wei, additional, Wright, George, additional, Kwei, Kevin, additional, Ping, Jerry, additional, Neuenburg, Jutta K., additional, and Staudt, Louis M., additional

Published

2021

14. Catalase reverses tumorigenicity in a malignant cell line by an epidermal growth factor receptor pathway

Author

Finch, Joanne S., Tome, Margaret E., Kwei, Kevin A., and Bowden, G. Tim

Published

2006

15. Rarity of B-Cell Receptor Pathway Mutations in Progression-Free Patients With Chronic Lymphocytic Leukemia (CLL) During First-Line Versus Relapsed/Refractory (R/R) Treatment With Ibrutinib

Author

Wiestner, Adrian, primary, Ghia, Paolo, additional, Byrd, John C., additional, Ahn, Inhye E, additional, Moreno, Carol, additional, O'Brien, Susan M., additional, Jones, Daniel, additional, Cheung, Leo W. K., additional, Chong, Elizabeth, additional, Kwei, Kevin, additional, Dean, James P., additional, James, Danelle F., additional, and Woyach, Jennifer A., additional

Published

2020

16. Outcomes of First-Line Ibrutinib in Patients with Chronic Lymphocytic Leukemia/Small Lymphocytic Lymphoma (CLL/SLL) and High-Risk Genomic Features with up to 6.5 Years Follow-up: Integrated Analysis of Two Phase 3 Studies (RESONATE-2 and iLLUMINATE)

Author

Burger, Jan A., primary, Robak, Tadeusz, additional, Demirkan, Fatih, additional, Bairey, Osnat, additional, Moreno, Carol, additional, Simpson, David, additional, Munir, Talha, additional, Stevens, Don A., additional, Dai, Sandra, additional, Cheung, Leo W. K., additional, Kwei, Kevin, additional, Lal, Indu, additional, Hsu, Emily, additional, Kipps, Thomas J., additional, and Tedeschi, Alessandra, additional

Published

2020

17. Transcriptional Repression of Catalase in Mouse Skin Tumor Progression

Author

Kwei, Kevin A., Finch, Joanne S., Thompson, Eric J., and Bowden, G. Tim

Published

2004

18. A RE-INTRODUCED CATALASE TRANSGENE ACTS AS A TUMOR SUPPRESSOR IN A MALIGNANT CELL LINE: 499

Author

Finch, Joanne S., Kwei, Kevin A, Tome, Margaret E., and Bowden, Tim G.

Published

2004

19. REGULATED EXPRESSION OF CATALASE AND ITS EFFECTS ON REACTIVE OXYGEN SPECIES AND GROWTH IN A MALIGNANT CELL LINE: 185

Author

Finch, Joanne, Kwei, Kevin A., Sikorski, Ewa, and Bowden, G. Tim

Published

2003

20. Phase 2 Results of the iR2 Regimen (Ibrutinib, Lenalidomide, and Rituximab) in Patients with Relapsed/Refractory (R/R) Non-Germinal Center B Cell-like (Non-GCB) Diffuse Large B-Cell Lymphoma (DLBCL)

Author

Ramchandren, Radhakrishnan, primary, Johnson, Peter, primary, Ghosh, Nilanjan, primary, Ruan, Jia, primary, Ardeshna, Kirit M., primary, Johnson, Roderick, primary, Verhoef, Gregor, primary, Cunningham, David, primary, de Vos, Sven, primary, Kassam, Shireen, primary, Fayad, Luis, primary, Radford, John, primary, Bailly, Sarah, primary, Offner, Fritz, primary, Morgan, David, primary, Munoz, Javier, primary, Ping, Jerry, primary, Kwei, Kevin, primary, Eckert, Karl, primary, Neuenburg, Jutta K., primary, and Goy, Andre, primary

Published

2019

21. Safety and activity of ibrutinib in combination with durvalumab in patients with relapsed or refractory follicular lymphoma or diffuse large B‐cell lymphoma

Author

Herrera, Alex F., primary, Goy, Andre, additional, Mehta, Amitkumar, additional, Ramchandren, Radhakrishnan, additional, Pagel, John M., additional, Svoboda, Jakub, additional, Guan, Shanhong, additional, Hill, John S., additional, Kwei, Kevin, additional, Liu, Emily A., additional, and Phillips, Tycel, additional

Published

2019

22. Abstract 3833: Systematic evaluation of transcriptome sequencing shows comparable profiles for an exome-capture method for formalin-fixed, paraffin-embedded (FFPE) breast cancer tissues and the standard poly-A method for matched fresh frozen (FF) tissues

Author

Zhao, Xi, primary, Zavodovskaya, Marianna, additional, Zhuo, Luting, additional, Kwei, Kevin, additional, Guo, Xin, additional, Jiang, Zhaoshi, additional, Patterson, Scott D., additional, and Brachmann, Carrie B., additional

Published

2017

23. Abstract 4197: Interaction of B lymphoma cells with the microenvironment affects ibrutinib sensitivity

Author

Kuo, Hsu-Ping, primary, Hsieh, Sidney, additional, Sirisawad, Mint, additional, Chen, Chun-Te, additional, Cheung, Leo W., additional, Schweighofer, Karl J., additional, Hsu, Chia-Lin, additional, Fu, Chi-Ling, additional, Liu, Jing, additional, Wu, Shiquan, additional, Eckert, Karl, additional, Wang, Hugh, additional, Apatira, Mutiah, additional, Dhami, Kamaldeep, additional, Kwei, Kevin, additional, Hsu, Jeff, additional, and Chang, Betty Y., additional

Published

2017

24. Safety and activity of ibrutinib in combination with durvalumab in patients with relapsed or refractory follicular lymphoma or diffuse large B‐cell lymphoma.

Author

Herrera, Alex F., Goy, Andre, Mehta, Amitkumar, Ramchandren, Radhakrishnan, Pagel, John M., Svoboda, Jakub, Guan, Shanhong, Hill, John S., Kwei, Kevin, Liu, Emily A., and Phillips, Tycel

Published

2020

25. Recurrent rearrangements of the Myb/SANT-like DNA-binding domain containing 3 gene (MSANTD3) in salivary gland acinic cell carcinoma

Author

Barasch, Nicholas, primary, Gong, Xue, additional, Kwei, Kevin A., additional, Varma, Sushama, additional, Biscocho, Jewison, additional, Qu, Kunbin, additional, Xiao, Nan, additional, Lipsick, Joseph S., additional, Pelham, Robert J., additional, West, Robert B., additional, and Pollack, Jonathan R., additional

Published

2017

26. Circulating Cytokines and Markers of Iron Metabolism in Myelofibrosis Patients Treated with Momelotininb: Correlatives from the Ym-387-II Study

Author

Gupta, Vikas, primary, Mesa, Ruben A., additional, Deininger, Michael W, additional, Rivera, Candido E., additional, Sirhan, Shireen, additional, Verstovsek, Srdan, additional, Zhang, Yafeng, additional, Xiao, Yuanyuan, additional, Collins, Helen, additional, Kwei, Kevin, additional, Joshi, Adarsh, additional, and Brachmann, Carrie Baker, additional

Published

2015

27. Integrative Genomics Implicates EGFR as a Downstream Mediator in NKX2-1 Amplified Non-Small Cell Lung Cancer

Author

Clarke, Nicole, primary, Biscocho, Jewison, additional, Kwei, Kevin A., additional, Davidson, Jean M., additional, Sridhar, Sushmita, additional, Gong, Xue, additional, and Pollack, Jonathan R., additional

Published

2015

28. Ibrutinib Therapy in Patients with Relapsed/Refractory Marginal Zone Lymphoma: Analysis By Prior Rituximab Treatment and Baseline Mutations

Author

Chen, Robert, de Vos, Sven, Thieblemont, Catherine, Martin, Peter, Flowers, Christopher, Morschhauser, Franck, Collins, Graham, Ma, Shuo, Coleman, Morton, Peles, Shachar, Smith, Stephen D., Barrientos, Jacqueline C., Smith, Alina, Munneke, Brian, Wu, Shiquan, Cheung, Leo, Kwei, Kevin, Samakoglu, Selda, Arango-Hisijara, Israel, Dimery, Isaiah, and Noy, Ariela

Published

2017

29. Erratum: Corrigendum: Identification of recurrent SMO and BRAF mutations in ameloblastomas

Author

Sweeney, Robert T, primary, McClary, Andrew C, additional, Myers, Benjamin R, additional, Biscocho, Jewison, additional, Neahring, Lila, additional, Kwei, Kevin A, additional, Qu, Kunbin, additional, Gong, Xue, additional, Ng, Tony, additional, Jones, Carol D, additional, Varma, Sushama, additional, Odegaard, Justin I, additional, Sugiyama, Toshihiro, additional, Koyota, Souichi, additional, Rubin, Brian P, additional, Troxell, Megan L, additional, Pelham, Robert J, additional, Zehnder, James L, additional, Beachy, Philip A, additional, Pollack, Jonathan R, additional, and West, Robert B, additional

Published

2014

30. Abstract 2375: A method to identify copy number aberrations (CNAs) from whole exome sequence (WES) data and its application to multiple myeloma cell lines and patient samples

Author

Degenhardt, Jeremiah D., primary, Hoehn, Kenneth B., additional, Kwei, Kevin A., additional, Stephenson, Kristi, additional, Keats, Jonathan J., additional, Kirk, Chris J., additional, and Tuch, Brian B., additional

Published

2014

31. Abstract 898: Expression of immunoglobulin and its receptor are major determinants of multiple myeloma patient sensitivity to proteasome inhibitors

Author

Tuch, Brian B., primary, Loehr, Andrea, additional, Degenhardt, Jeremiah D., additional, Kwei, Kevin A., additional, Lowe, Eric, additional, Stephenson, Kristi, additional, Keats, Jonathan J., additional, and Kirk, Christopher J., additional

Published

2014

32. Abstract 3436: Ameloblastoma driver mutations revealed by next-generation sequencing of formalin-fixed paraffin-embedded specimens

Author

McClary, Andrew C., primary, Sweeney, Robert T., additional, Biscocho, Jewison, additional, Myers, Benjamin R., additional, Neahring, Lila, additional, Kwei, Kevin A., additional, Qu, Kunbin, additional, Gong, Xue, additional, Ng, Tony, additional, Jones, Carol D., additional, Varma, Sushama, additional, Odegaard, Justin I., additional, Rubin, Brian, additional, Troxell, Megan L., additional, Pelham, Robert J., additional, Zehnder, James L., additional, Beachy, Philip A., additional, Pollack, Jonathan R., additional, and West, Robert B., additional

Published

2014

33. Ameloblastoma driver mutations revealed by next‐generation sequencing of formalin‐fixed paraffin‐embedded specimens (1048.18)

Author

Pollack, Jonathan, primary, McClary, Andrew, additional, Sweeney, Robert, additional, Biscocho, Jewison, additional, Myers, Benjamin, additional, Neahring, Lila, additional, Kwei, Kevin, additional, Qu, Kunbin, additional, Gong, Xu, additional, Ng, Tony, additional, Jones, Carol, additional, Varma, Sushama, additional, Odegaard, Justin, additional, Rubin, Brian, additional, Troxell, Megan, additional, Pelham, Robert, additional, Zehnder, James, additional, Beachy, Philip, additional, and West, Robert, additional

Published

2014

34. A Method To Identify Copy Number Aberrations (CNAs) From Whole Exome Sequence (WES) Data and Its Application To Multiple Myeloma Cell Lines and Patient Samples

Author

Degenhardt, Jeremiah D, primary, Hoehn, Kenneth B, additional, Kwei, Kevin A, additional, Keats, Jonathan J, additional, Kirk, Christopher J., additional, and Tuch, Brian B, additional

Published

2013

35. Immunoglobulin Expression Is a Major Determinant Of Patient Sensitivity To Proteasome Inhibitors

Author

Tuch, Brian B, primary, Loehr, Andrea, additional, Degenhardt, Jeremiah D, additional, Kwei, Kevin A, additional, Keats, Jonathan J, additional, and Kirk, Christopher J., additional

Published

2013

36. Development Of Methods To Perform Next Generation Sequencing (NGS)-Based Genomics Studies On Multiple Myeloma Clinical Samples

Author

Keats, Jonathan J, primary, Kwei, Kevin A, additional, Degenhardt, Jeremiah D, additional, Allen, Kristi, additional, Kirk, Christopher J., additional, and Tuch, Brian B, additional

Published

2013

37. Modulators of Sensitivity and Resistance to Inhibition of PI3K Identified in a Pharmacogenomic Screen of the NCI-60 Human Tumor Cell Line Collection

Author

Kwei, Kevin A., primary, Baker, Joffre B., additional, and Pelham, Robert J., additional

Published

2012

38. Molecular mechanisms of tumor progression in mouse skin keratinocytes

Author

Kwei, Kevin Anthony and Kwei, Kevin Anthony

Abstract

Our laboratory had previously developed an in vitro tumor progression model which demonstrated that elevation of Reactive Oxygen Species (ROS) played a functional role in the development and maintenance of malignantly transformed mouse skin keratinocytes. The elevation of ROS levels were attributed to the repression of the anti-oxidant enzyme catalase. We hypothesized that repression of catalase, a potential tumor suppressor gene, led to the elevation of hydrogen peroxide which functions as a secondary messenger to active mitogenic signaling in the malignant cells. The first goal of these studies was to further characterize the repression of catalase in vivo. Using tumor samples generated by the mouse skin chemical carcinogenesis protocol, we determined that papillomas expressed higher levels of catalase protein and message than carcinomas. These results recapitulated the observations we made in the in vitro tumor progression model. The next goal was to determine the mechanism(s) behind the repression of catalase. Nuclear run-on analysis showed that catalase repression in the malignantly transformed cells was dependent on transcription. Results from luciferase reporter assays indicated that malignant cells have lower catalase promoter activities than benign papilloma cells, in part through the Wilm's tumor suppressor (WT1) binding site within the proximal promoter region. We concluded that WT1 element acts as a transcriptional repressor of catalase in this tumor progression model. The second part of this dissertation is focused on the role of the Rac1 signaling in tumor progression. Rac1 has been shown to activate NADPH oxidase to produce superoxide, potentially contributing to the elevation of ROS. We found that conditional expression of a dominant negative Rac1 was able to decrease multiple markers of malignancy including: growth, migration and invasion potential. In addition, these phenotypic changes were accompanied by a decrease in mitogenic signaling. Furtherm

Published

2004

39. SMURF1 Amplification Promotes Invasiveness in Pancreatic Cancer

Author

Kwei, Kevin A., primary, Shain, A. Hunter, additional, Bair, Ryan, additional, Montgomery, Kelli, additional, Karikari, Collins A., additional, van de Rijn, Matt, additional, Hidalgo, Manuel, additional, Maitra, Anirban, additional, Bashyam, Murali D., additional, and Pollack, Jonathan R., additional

Published

2011

40. Molecular Profiling of Breast Cancer Cell Lines Defines Relevant Tumor Models and Provides a Resource for Cancer Gene Discovery

Author

Kao, Jessica, primary, Salari, Keyan, additional, Bocanegra, Melanie, additional, Choi, Yoon-La, additional, Girard, Luc, additional, Gandhi, Jeet, additional, Kwei, Kevin A., additional, Hernandez-Boussard, Tina, additional, Wang, Pei, additional, Gazdar, Adi F., additional, Minna, John D., additional, and Pollack, Jonathan R., additional

Published

2009

41. CAMK1Damplification implicated in epithelial-mesenchymal transition in basal-like breast cancer

Author

Bergamaschi, Anna, primary, Kim, Young H., additional, Kwei, Kevin A., additional, La Choi, Yoon, additional, Bocanegra, Melanie, additional, Langerød, Anita, additional, Han, Wonshik, additional, Noh, Dong-Young, additional, Huntsman, David G., additional, Jeffrey, Stefanie S., additional, Børresen-Dale, Anne-Lise, additional, and Pollack, Jonathan R., additional

Published

2008

42. Genomic Profiling Identifies GATA6 as a Candidate Oncogene Amplified in Pancreatobiliary Cancer

Author

Kwei, Kevin A., primary, Bashyam, Murali D., additional, Kao, Jessica, additional, Ratheesh, Raman, additional, Reddy, Edumakanti C., additional, Kim, Young H., additional, Montgomery, Kelli, additional, Giacomini, Craig P., additional, Choi, Yoon-La, additional, Chatterjee, Sreejata, additional, Karikari, Collins A., additional, Salari, Keyan, additional, Wang, Pei, additional, Hernandez-Boussard, Tina, additional, Swarnalata, Gowrishankar, additional, van de Rijn, Matt, additional, Maitra, Anirban, additional, and Pollack, Jonathan R., additional

Published

2008

43. Integrin A6 Cleavage in Mouse Skin Tumors

Author

Cress, Anne E., primary, Demetriou, Manolis C., additional, Kwei, Kevin A., additional, Powell, Marianne B., additional, Nagle, Raymond B., additional, and Bowden, G. Tim, additional

Published

2008

44. The role of Rac1 in maintaining malignant phenotype of mouse skin tumor cells

Author

Kwei, Kevin A., primary, Finch, Joanne S., additional, Ranger-Moore, James, additional, and Bowden, G. Tim, additional

Published

2006

45. Elevated basal reactive oxygen species and phospho-Akt in murine keratinocytes resistant to ultraviolet B-induced apoptosis

Author

Butts, Brent D., primary, Kwei, Kevin A., additional, Bowden, G. Tim, additional, and Briehl, Margaret M., additional

Published

2003

46. Attenuation of catalase activity in the malignant phenotype plays a functional role in an in vitro model for tumor progression

Author

Gupta, Ashok, primary, Butts, Brent, additional, Kwei, Kevin A., additional, Dvorakova, Katerina, additional, Stratton, Steven P., additional, Briehl, Margaret M., additional, and Bowden, G.Tim, additional

Published

2001

47. Phase 2 Results of the iR2Regimen (Ibrutinib, Lenalidomide, and Rituximab) in Patients with Relapsed/Refractory (R/R) Non-Germinal Center B Cell-like (Non-GCB) Diffuse Large B-Cell Lymphoma (DLBCL)

Author

Ramchandren, Radhakrishnan, Johnson, Peter, Ghosh, Nilanjan, Ruan, Jia, Ardeshna, Kirit M., Johnson, Roderick, Verhoef, Gregor, Cunningham, David, de Vos, Sven, Kassam, Shireen, Fayad, Luis, Radford, John, Bailly, Sarah, Offner, Fritz, Morgan, David, Munoz, Javier, Ping, Jerry, Kwei, Kevin, Eckert, Karl, Neuenburg, Jutta K., and Goy, Andre

Abstract

Background:DLBCL is an aggressive non-Hodgkin lymphoma (NHL) with poor outcomes in the R/R setting; overall survival (OS) is 28% at 1 year and 20% at 2 years in refractory patients (Crump, Blood2017). Outcomes are particularly poor for patients ineligible for stem cell transplant (SCT). Ibrutinib is the only once-daily inhibitor of Bruton's tyrosine kinase and is approved for the treatment of various B-cell malignancies. Based on preclinical models, ibrutinib and lenalidomide, an immunomodulator that downregulates the MYD88 pathway, may synergize when combined (Yang, Cancer Cell2012). Rituximab, an anti-CD20 antibody, has shown activity combined with ibrutinib in NHL (Wang, Lancet Onc2016). PCYC-1123 is a multicenter, open-label phase 1b/2 study (NCT02077166) evaluating the combination of ibrutinib, lenalidomide, and rituximab (iR2) in R/R DLBCL.

Published

2019

48. Corrigendum: Identification of recurrent SMO and BRAF mutations in ameloblastomas.

Author

Sweeney, Robert T, McClary, Andrew C, Myers, Benjamin R, Biscocho, Jewison, Neahring, Lila, Kwei, Kevin A, Qu, Kunbin, Gong, Xue, Ng, Tony, Jones, Carol D, Varma, Sushama, Odegaard, Justin I, Sugiyama, Toshihiro, Koyota, Souichi, Rubin, Brian P, Troxell, Megan L, Pelham, Robert J, Zehnder, James L, Beachy, Philip A, and Pollack, Jonathan R

Subjects

AMELOBLASTOMA, BRAF genes

Abstract

A correction to the article “Identification of recurrent SMO and BRAF mutations in ameloblastomas" that was published in the 25 May, 2014 online issue is presented.

Published

2015

49. Integrin A6 Cleavage in Mouse Skin Tumors.

Author

Demetriou MC, Kwei KA, Powell MB, Nagle RB, Bowden GT, and Cress AE

Abstract

We have previously identified a structural variant of the α6 integrin (Laminin receptor) called α6p. The α6p variant is a 70 kDa form of the full-length α6 integrin (140 kDa) that remains paired with either the β1 or β4 subunit on the cell surface. α6p is produced by urokinase-type plasminogen activator (uPA), which removes the extracellular β-barrel domain while the receptor is on the cell surface. The α6p integrin was present in human prostate cancer tissue but not in normal tissue and the cleavage of the α6 integrin extracellular domain promotes tumor cell invasion and migration on laminin. The objective of the present study was to determine whether the α6p integrin is observed in other models of carcinogenesis. Our results indicate detectable low levels of α6p in normal mouse skin, and comparatively elevated levels in mouse papillomas and squamous cell carcinomas induced by DMBA, TPA and MNNG treatments. Furthermore, we have found that α6p was present at high levels in skin melanomas of transgenic mice that over express activated Ha-ras under the control of the tyrosinase promoter. Finally, subcutaneous injection into athymic nude mice of a malignant mouse keratinocyte derived cell line (6M90) that is α6p negative, results in the development of tumors that contain α6p integrin. The latter results indicate that α6p is induced in vivo suggesting that the tumor microenvironment plays a major role in the production of α6p. Taken together, these data suggest that the cell surface cleavage of the α6 integrin may be a novel mechanism of integrin regulation and might be an important step during skin tissue remodeling and during carcinogenesis.

Published

2008